庞贝病、法布雷病和黏多糖贮积症 IIIB 溶酶体贮积病的小鼠模型中的主动脉病变。
Aortopathies in mouse models of Pompe, Fabry and Mucopolysaccharidosis IIIB lysosomal storage diseases.
机构信息
Department of Radiology, University of Campania "L. Vanvitelli", Naples, Italy.
Department of Translational Medical Sciences, Federico II University, Naples, Italy.
出版信息
PLoS One. 2020 May 19;15(5):e0233050. doi: 10.1371/journal.pone.0233050. eCollection 2020.
INTRODUCTION
Lysosomal storage diseases (LSDs) are rare inherited metabolic diseases characterized by an abnormal accumulation of various toxic materials in the cells as a result of enzyme deficiencies leading to tissue and organ damage. Among clinical manifestations, cardiac diseases are particularly important in Pompe glycogen storage diseases (PD), in glycosphingolipidosis Fabry disease (FD), and mucopolysaccharidoses (MPS). Here, we evaluated the occurrence of aortopathy in knock out (KO) mouse models of three different LSDs, including PD, FD, and MPS IIIB.
METHODS
We measured the aortic diameters in 15 KO male mice, 5 for each LSD: 5 GLA-/- mice for FD, 5 NAGLU-/- mice for MPS IIIB, 5 GAA-/- mice for PD, and 15 wild type (WT) mice: 5 for each strain. In order to compare the aortic parameters between KO and WT mice deriving from the same colonies, different diameters were echocardiographically measured: aortic annulus, aortic sinus, sino-tubular junction, ascending aorta, aortic arch and descending aorta. Storage material content and aortic defects of the KO mice were also analyzed by histology, when available.
RESULTS
Compared to their correspondent WT mice: GAA-/- mice showed greater diameters of ascending aorta (1.61mm vs. 1.11mm, p-value = 0.01) and descending aorta (1.17mm vs 1.02mm, p-value 0.04); GLA-/- mice showed greater diameters of aortic annulus (1.35mm vs. 1.22mm, p-value = 0.01), sinus of Valsalva (1.6mm vs. 1.38mm, p-value<0.01), ascending aorta (1.57mm vs. 1.34mm, p-value<0.01), aortic arch (1.36mm vs. 1.22mm, p-value = 0.03) and descending aorta (1.29mm vs. 1.11mm, p-value<0.01); NAGLU-/- mice showed greater diameters of sinus of Valsalva (1.46mm vs. 1.31mm, p-value = 0.05), ascending aorta (1.42mm vs. 1.29mm, p-value<0.01), aortic arch (1.34mm vs. 1.28mm, p-value<0.01) and descending aorta (1.18mm vs. 1.1mm, p-value 0.01).
CONCLUSIONS
We evaluated for the first time the aortic diameters in 3 LSD mouse models and identified different aortopathy patterns, in concordance with recent human findings. Our results are relevant in view of using KO mouse models for efficiently testing the efficacy of new therapies on distinct cardiovascular aspects of LSDs.
简介
溶酶体贮积症(LSD)是一种罕见的遗传性代谢疾病,其特征是由于酶缺乏导致各种有毒物质在细胞内异常积累,从而导致组织和器官损伤。在临床表现中,心脏疾病在庞贝氏糖原贮积症(PD)、法布里病(FD)的糖脂沉积病和黏多糖贮积症(MPS)中尤为重要。在这里,我们评估了三种不同 LSD 的敲除(KO)小鼠模型中的主动脉病变,包括 PD、FD 和 MPS IIIB。
方法
我们测量了 15 只 KO 雄性小鼠的主动脉直径,每种 LSD 有 5 只:5 只 GLA-/- 小鼠用于 FD,5 只 NAGLU-/- 小鼠用于 MPS IIIB,5 只 GAA-/- 小鼠用于 PD,还有 15 只野生型(WT)小鼠:每只品系 5 只。为了比较来自同一品系的 KO 和 WT 小鼠的主动脉参数,我们通过超声心动图测量了不同的直径:主动脉瓣环、主动脉窦、窦管交界处、升主动脉、主动脉弓和降主动脉。当有组织学资料时,我们还分析了 KO 小鼠的储存物质含量和主动脉缺陷。
结果
与相应的 WT 小鼠相比:GAA-/- 小鼠的升主动脉(1.61mm 比 1.11mm,p 值=0.01)和降主动脉(1.17mm 比 1.02mm,p 值=0.04)直径较大;GLA-/- 小鼠的主动脉瓣环(1.35mm 比 1.22mm,p 值=0.01)、瓦尔萨尔瓦窦(1.6mm 比 1.38mm,p 值<0.01)、升主动脉(1.57mm 比 1.34mm,p 值<0.01)、主动脉弓(1.36mm 比 1.22mm,p 值=0.03)和降主动脉(1.29mm 比 1.11mm,p 值<0.01)直径较大;NAGLU-/- 小鼠的瓦尔萨尔瓦窦(1.46mm 比 1.31mm,p 值=0.05)、升主动脉(1.42mm 比 1.29mm,p 值<0.01)、主动脉弓(1.34mm 比 1.28mm,p 值<0.01)和降主动脉(1.18mm 比 1.1mm,p 值 0.01)直径较大。
结论
我们首次在 3 种 LSD 小鼠模型中评估了主动脉直径,并根据最近的人类发现确定了不同的主动脉病变模式。鉴于使用 KO 小鼠模型有效地测试新疗法对 LSD 不同心血管方面的疗效,我们的研究结果具有相关性。
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